Biometric and Psychometric Remote Monitoring and Cardiovascular Risk Biomarkers in Ischemic Heart Disease

Author:

Shufelt Chrisandra L.1ORCID,Kim Andy1ORCID,Joung Sandy1ORCID,Barsky Lili1,Arnold Corey2ORCID,Cheng Susan1ORCID,Dhawan Shivani1,Fuller Garth3,Speier William2ORCID,Lopez Mayra3ORCID,Mastali Mitra14,Mouapi Kelly14,van den Broek Irene14,Wei Janet1,Spiegel Brennan2,Van Eyk Jennifer E.14,Bairey-Merz C. Noel1ORCID

Affiliation:

1. Barbra Streisand Women’s Heart Center Smidt Heart Institute Cedars‐Sinai Medical Center Los Angeles CA

2. Medical Imaging and Informatics Group University of California Los Angeles CA

3. Cedars‐Sinai Center for Outcomes Research and Education (CS‐CORE) Los Angeles CA

4. Advanced Clinical Biosystems Research Institute Cedars‐Sinai Smidt Heart Institute Cedars‐Sinai Medical Center Los Angeles CA

Abstract

Background Patients with stable ischemic heart disease represent a heterogeneous population at variable risk for major adverse cardiac events (MACE). Because MACE typically occurs outside the hospital, we studied whether biometric and psychometric remote patient monitoring are associated with MACE risk biomarkers. Methods and Results In 198 patients with stable ischemic heart disease (mean age 65±11 years, 60% women), we evaluated baseline measures, including biometric (FitBit 2) and psychometric (acquired via smartphone‐administered patient‐reported outcomes) remote monitoring, in the PRE‐MACE (Prediction, Risk, and Evaluation of Major Adverse Cardiac Events) study. In multivariable adjusted regression analyses, we examined the association of these measures with biomarkers of MACE risk, including NT‐proBNP (N‐terminal pro‐b‐type natriuretic peptide), u‐hs‐cTnI (ultra‐high sensitivity cardiac‐specific troponin I), and hs‐CRP (high‐sensitivity C‐reactive) protein. Both biometric and psychometric measures were associated with NT‐proBNP. Specifically, step count, heart rate, physical activity, global health score, and physical function score were all inversely related, whereas physical limitation score was directly related ( P ≤0.05 for all). However, only biometric measures (step count and heart rate) were associated with u‐hs‐cTnI (inversely related, P <0.05), while only the psychometric measures of physical limitation were associated with hs‐CRP (directly related, P ≤0.05). Conclusions In stable ischemic heart disease patients, remotely monitored measures were associated with MACE risk biomarkers. Both biometric and psychometric measures were related to NT‐proBNP. In contrast, biometric measures were uniquely related to u‐hs‐cTnI, while psychometric indices were uniquely related to hs‐CRP. Further investigation could assess the predictive value of these metrics for MACE in ischemic heart disease.

Publisher

Ovid Technologies (Wolters Kluwer Health)

Subject

Cardiology and Cardiovascular Medicine

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